A member of the gut mycobiota modulates host purine metabolism exacerbating colitis in mice

Tyson R. Chiaro; Ray Soto; W. Zac Stephens; Jason L. Kubinak; Charisse Petersen; Lasha Gogokhia; Rickesha Bell; Julio C. Delgado; James Cox; Warren Voth; Jessica Brown; David J. Stillman; Ryan M. O'Connell; Anne E. Tebo; June L. Round

doi:10.1126/scitranslmed.aaf9044

A member of the gut mycobiota modulates host purine metabolism exacerbating colitis in mice

Tyson R. Chiaro
, Ray Soto
, W. Zac Stephens
, Jason L. Kubinak
, Charisse Petersen
, Lasha Gogokhia
, Rickesha Bell
, Julio C. Delgado
, James Cox
, Warren Voth
, Jessica Brown
, David J. Stillman
, Ryan M. O'Connell
, Anne E. Tebo
, June L. Round

Gastroenterology and Hepatology

University of Utah

Research output: Contribution to journal › Article › peer-review

216 Scopus citations

Abstract

The commensal microbiota has an important impact on host health, which is only beginning to be elucidated. Despite the presence of fungal, archaeal, and viral members, most studies have focused solely on the bacterial microbiota. Antibodies against the yeast Saccharomyces cerevisiae are found in some patients with Crohn's disease (CD), suggesting that the mycobiota may contribute to disease severity. We report that S. cerevisiae exacerbated intestinal disease in a mouse model of colitis and increased gut barrier permeability. Transcriptome analysis of colon tissue from germ-free mice inoculated with S. cerevisiae or another fungus, Rhodotorula aurantiaca, revealed that S. cerevisiae colonization affected the intestinal barrier and host metabolism. A fecal metabolomics screen of germ-free animals demonstrated that S. cerevisiae colonization enhanced host purine metabolism, leading to an increase in uric acid production. Treatment with uric acid alone worsened disease and increased gut permeability. Allopurinol, a clinical drug used to reduce uric acid, ameliorated colitis induced by S. cerevisiae in mice. In addition, we found a positive correlation between elevated uric acid and anti-yeast antibodies in human sera. Thus, yeast in the gut may be able to potentiate metabolite production that negatively affects the course of inflammatory bowel disease.

Original language	English
Article number	eaaf9044
Journal	Science Translational Medicine
Volume	9
Issue number	380
DOIs	https://doi.org/10.1126/scitranslmed.aaf9044
State	Published - Mar 8 2017

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Chiaro, T. R., Soto, R., Stephens, W. Z., Kubinak, J. L., Petersen, C., Gogokhia, L., Bell, R., Delgado, J. C., Cox, J., Voth, W., Brown, J., Stillman, D. J., O'Connell, R. M., Tebo, A. E., & Round, J. L. (2017). A member of the gut mycobiota modulates host purine metabolism exacerbating colitis in mice. Science Translational Medicine, 9(380), Article eaaf9044. https://doi.org/10.1126/scitranslmed.aaf9044

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title = "A member of the gut mycobiota modulates host purine metabolism exacerbating colitis in mice",

abstract = "The commensal microbiota has an important impact on host health, which is only beginning to be elucidated. Despite the presence of fungal, archaeal, and viral members, most studies have focused solely on the bacterial microbiota. Antibodies against the yeast Saccharomyces cerevisiae are found in some patients with Crohn's disease (CD), suggesting that the mycobiota may contribute to disease severity. We report that S. cerevisiae exacerbated intestinal disease in a mouse model of colitis and increased gut barrier permeability. Transcriptome analysis of colon tissue from germ-free mice inoculated with S. cerevisiae or another fungus, Rhodotorula aurantiaca, revealed that S. cerevisiae colonization affected the intestinal barrier and host metabolism. A fecal metabolomics screen of germ-free animals demonstrated that S. cerevisiae colonization enhanced host purine metabolism, leading to an increase in uric acid production. Treatment with uric acid alone worsened disease and increased gut permeability. Allopurinol, a clinical drug used to reduce uric acid, ameliorated colitis induced by S. cerevisiae in mice. In addition, we found a positive correlation between elevated uric acid and anti-yeast antibodies in human sera. Thus, yeast in the gut may be able to potentiate metabolite production that negatively affects the course of inflammatory bowel disease.",

author = "Chiaro, \{Tyson R.\} and Ray Soto and Stephens, \{W. Zac\} and Kubinak, \{Jason L.\} and Charisse Petersen and Lasha Gogokhia and Rickesha Bell and Delgado, \{Julio C.\} and James Cox and Warren Voth and Jessica Brown and Stillman, \{David J.\} and O'Connell, \{Ryan M.\} and Tebo, \{Anne E.\} and Round, \{June L.\}",

note = "Publisher Copyright: {\textcopyright} 2017 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science.",

year = "2017",

month = mar,

day = "8",

doi = "10.1126/scitranslmed.aaf9044",

language = "English",

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Chiaro, TR, Soto, R, Stephens, WZ, Kubinak, JL, Petersen, C, Gogokhia, L, Bell, R, Delgado, JC, Cox, J, Voth, W, Brown, J, Stillman, DJ, O'Connell, RM, Tebo, AE & Round, JL 2017, 'A member of the gut mycobiota modulates host purine metabolism exacerbating colitis in mice', Science Translational Medicine, vol. 9, no. 380, eaaf9044. https://doi.org/10.1126/scitranslmed.aaf9044

TY - JOUR

T1 - A member of the gut mycobiota modulates host purine metabolism exacerbating colitis in mice

AU - Chiaro, Tyson R.

AU - Soto, Ray

AU - Stephens, W. Zac

AU - Kubinak, Jason L.

AU - Petersen, Charisse

AU - Gogokhia, Lasha

AU - Bell, Rickesha

AU - Delgado, Julio C.

AU - Cox, James

AU - Voth, Warren

AU - Brown, Jessica

AU - Stillman, David J.

AU - O'Connell, Ryan M.

AU - Tebo, Anne E.

AU - Round, June L.

PY - 2017/3/8

Y1 - 2017/3/8

N2 - The commensal microbiota has an important impact on host health, which is only beginning to be elucidated. Despite the presence of fungal, archaeal, and viral members, most studies have focused solely on the bacterial microbiota. Antibodies against the yeast Saccharomyces cerevisiae are found in some patients with Crohn's disease (CD), suggesting that the mycobiota may contribute to disease severity. We report that S. cerevisiae exacerbated intestinal disease in a mouse model of colitis and increased gut barrier permeability. Transcriptome analysis of colon tissue from germ-free mice inoculated with S. cerevisiae or another fungus, Rhodotorula aurantiaca, revealed that S. cerevisiae colonization affected the intestinal barrier and host metabolism. A fecal metabolomics screen of germ-free animals demonstrated that S. cerevisiae colonization enhanced host purine metabolism, leading to an increase in uric acid production. Treatment with uric acid alone worsened disease and increased gut permeability. Allopurinol, a clinical drug used to reduce uric acid, ameliorated colitis induced by S. cerevisiae in mice. In addition, we found a positive correlation between elevated uric acid and anti-yeast antibodies in human sera. Thus, yeast in the gut may be able to potentiate metabolite production that negatively affects the course of inflammatory bowel disease.

AB - The commensal microbiota has an important impact on host health, which is only beginning to be elucidated. Despite the presence of fungal, archaeal, and viral members, most studies have focused solely on the bacterial microbiota. Antibodies against the yeast Saccharomyces cerevisiae are found in some patients with Crohn's disease (CD), suggesting that the mycobiota may contribute to disease severity. We report that S. cerevisiae exacerbated intestinal disease in a mouse model of colitis and increased gut barrier permeability. Transcriptome analysis of colon tissue from germ-free mice inoculated with S. cerevisiae or another fungus, Rhodotorula aurantiaca, revealed that S. cerevisiae colonization affected the intestinal barrier and host metabolism. A fecal metabolomics screen of germ-free animals demonstrated that S. cerevisiae colonization enhanced host purine metabolism, leading to an increase in uric acid production. Treatment with uric acid alone worsened disease and increased gut permeability. Allopurinol, a clinical drug used to reduce uric acid, ameliorated colitis induced by S. cerevisiae in mice. In addition, we found a positive correlation between elevated uric acid and anti-yeast antibodies in human sera. Thus, yeast in the gut may be able to potentiate metabolite production that negatively affects the course of inflammatory bowel disease.

UR - https://www.scopus.com/pages/publications/85014918566

U2 - 10.1126/scitranslmed.aaf9044

DO - 10.1126/scitranslmed.aaf9044

M3 - Article

C2 - 28275154

AN - SCOPUS:85014918566

SN - 1946-6234

VL - 9

JO - Science Translational Medicine

JF - Science Translational Medicine

IS - 380

M1 - eaaf9044

ER -

A member of the gut mycobiota modulates host purine metabolism exacerbating colitis in mice

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